A HIV vaccine cannot consist of attenuated (a virus altered to become harmless or less virulent) but actively replicating (live) HIV, due to the possibility it would become harmful or more virulent.

Using dead whole virus (like the polio vaccine) might also be dangerous because you could never be sure every virus particle had been killed.

HIV is a retrovirus which integrates its genome into the human genome. In this way, it is able to hide from the immune system. Scientists have had limited success in developing a vaccine against a retrovirus like HIV. Retroviruses have a relatively high rate of mutation. HIV viruses replicate very quickly causing the development of viruses that differ from the vaccine strain. This means that any vaccine has a small window of time to prevent infection and would have to be extremely effective.

The earliest known case of infection with HIV-1 in a human was detected in a blood sample collected in 1959 from a man in Kinshasa, Democratic Republic of the Congo. (How he became infected is not known.) Genetic analysis of this blood sample suggested that HIV-1 may have stemmed from a single virus in the late 1940s or early 1950s.— The Aids Institute

Not Really an HIV Vaccine

A team at Scripps Research Institute, including Micheal Farzan, has discovered a protein on the surface of white blood cells that binds to a HIV virus in two places at the same time. These receptor sites are what the virus uses to attach to the receptors CD4 and CCR5.

With the protein, called eCD4-lg attached, the virus can’t change the position of its receptors. Thus it can’t escape. In this tight hold, the protein blocks the virus from entering the T-lymphocyte cells. If it can’t penetrate the cell, it can’t multiply.

Not an HIV Vaccine but a Vaccine Alternative

This miracle is not a vaccine but a vaccine alternative. In non-human tests it is effective against HIV-1, HIV-2 and SIV. It has worked against huge viral loads and has stayed effective for at least 8 months after injection. It works so well that this treatment acts like a vaccine giving long-term protection.

How Does the HIV “Vaccine” Work?

Just how do you get this protein, eCD4-lg, into the body and get it to give long-lasting protection like a vaccine? Gene therapy is the answer my friends.

In a nutshell, gene therapy uses genes to treat or prevent disease. Instead of drugs or surgery, a gene is inserted into a patient’s cells usually using a virus to deliver the gene.

And so it is with the HIV vaccine: the gene for the protein, eCD4-lg, is inserted into a weakened, harmless virus. The virus targets a patient’s healthy muscle cells inserting the gene into those cells. The normal activity of those muscle cells now produces the HIV-blocking protein, eCD4-lg, which is continually pumped into the bloodstream.

In monkeys, this vaccine provided protection for 34 weeks. It is strongly thought that the research team will be able to tweak the vaccine to give even longer protection up to years or even decades.

Human Trials for the HIV Vaccine

Human trials will be conducted, in one to two years, by Michael Farzan and colleagues funded by the Bill and Melinda Gates Foundation. Initially, the human trials will use the protein inhibitor, eCD4-lg, alone to test its ability to suppress the virus in affected people.

At the same time, this grant will also be used to improve the delivery mechanism of the gene coding this protein – the weakened virus.

It looks like a real solution to the HIV epidemic is around the corner. Is it a real vaccine? No, it is not. But, through the ever advancing miracle of gene therapy, perhaps an even better solution is on the horizon. Vaccines are very type specific meaning they will prime your immune system for only one strain of the virus. HIV comes in many strains.

This therapy promises protection against all strains of HIV by providing the body with the instructions to make a protein that affects one factor in how they attach to the white blood cells, that has remained unchanged in all strains.

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